Literature DB >> 25428879

Human noroviruses' fondness for histo-blood group antigens.

Bishal K Singh1, Mila M Leuthold1, Grant S Hansman2.   

Abstract

UNLABELLED: Human noroviruses are the dominant cause of outbreaks of gastroenteritis around the world. Human noroviruses interact with the polymorphic human histo-blood group antigens (HBGAs), and this interaction is thought to be important for infection. Indeed, synthetic HBGAs or HBGA-expressing enteric bacteria were shown to enhance norovirus infection in B cells. A number of studies have found a possible relationship between HBGA type and norovirus susceptibility. The genogroup II, genotype 4 (GII.4) noroviruses are the dominant cluster, evolve every other year, and are thought to modify their binding interactions with different HBGA types. Here we show high-resolution X-ray crystal structures of the capsid protruding (P) domains from epidemic GII.4 variants from 2004, 2006, and 2012, cocrystallized with a panel of HBGA types (H type 2, Lewis Y, Lewis B, Lewis A, Lewis X, A type, and B type). Many of the HBGA binding interactions were found to be complex, involving capsid loop movements, alternative HBGA conformations, and HBGA rotations. We showed that a loop (residues 391 to 395) was elegantly repositioned to allow for Lewis Y binding. This loop was also slightly shifted to provide direct hydrogen- and water-mediated bonds with Lewis B. We considered that the flexible loop modulated Lewis HBGA binding. The GII.4 noroviruses have dominated outbreaks over the past decade, which may be explained by their exquisite HBGA binding mechanisms, their fondness for Lewis HBGAs, and their temporal amino acid modifications. IMPORTANCE: Our data provide a comprehensive picture of GII.4 P domain and HBGA binding interactions. The exceptionally high resolutions of our X-ray crystal structures allowed us to accurately recognize novel GII.4 P domain interactions with numerous HBGA types. We showed that the GII.4 P domain-HBGA interactions involved complex binding mechanisms that were not previously observed in norovirus structural studies. Many of the GII.4 P domain-HBGA interactions we identified were negative in earlier enzyme-linked immunosorbent assay (ELISA)-based studies. Altogether, our data show that the GII.4 norovirus P domains can accommodate numerous HBGA types.
Copyright © 2015, American Society for Microbiology. All Rights Reserved.

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Year:  2014        PMID: 25428879      PMCID: PMC4338890          DOI: 10.1128/JVI.02968-14

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  35 in total

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2.  Emergence of new pandemic GII.4 Sydney norovirus strain correlates with escape from herd immunity.

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Journal:  J Infect Dis       Date:  2013-08-01       Impact factor: 5.226

3.  Norovirus-host interaction: multi-selections by human histo-blood group antigens.

Authors:  Ming Tan; Xi Jiang
Journal:  Trends Microbiol       Date:  2011-06-24       Impact factor: 17.079

4.  Enteric bacteria promote human and mouse norovirus infection of B cells.

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9.  Analysis of amino acid variation in the P2 domain of the GII-4 norovirus VP1 protein reveals putative variant-specific epitopes.

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  46 in total

1.  Structural Evolution of the Emerging 2014-2015 GII.17 Noroviruses.

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Journal:  J Virol       Date:  2015-12-23       Impact factor: 5.103

2.  Avidity of α-fucose on human milk oligosaccharides and blood group-unrelated oligo/polyfucoses is essential for potent norovirus-binding targets.

Authors:  Franz-Georg Hanisch; Grant S Hansman; Vasily Morozov; Clemens Kunz; Horst Schroten
Journal:  J Biol Chem       Date:  2018-06-01       Impact factor: 5.157

Review 3.  Current tools for norovirus drug discovery.

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Journal:  Expert Opin Drug Discov       Date:  2016-05-02       Impact factor: 6.098

4.  Production of Human Norovirus Protruding Domains in E. coli for X-ray Crystallography.

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Journal:  J Vis Exp       Date:  2016-04-19       Impact factor: 1.355

5.  Epitope mapping of histo blood group antigens bound to norovirus VLPs using STD NMR experiments reveals fine details of molecular recognition.

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Journal:  Glycoconj J       Date:  2017-08-19       Impact factor: 2.916

6.  Structural basis for norovirus neutralization by an HBGA blocking human IgA antibody.

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7.  Nanobody binding to a conserved epitope promotes norovirus particle disassembly.

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8.  Atomic Structure of the Murine Norovirus Protruding Domain and Soluble CD300lf Receptor Complex.

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9.  Structural Basis for Human Norovirus Capsid Binding to Bile Acids.

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Journal:  J Virol       Date:  2019-01-04       Impact factor: 5.103

Review 10.  Human Norovirus Interactions with Histo-Blood Group Antigens and Human Milk Oligosaccharides.

Authors:  Horst Schroten; Franz-Georg Hanisch; Grant S Hansman
Journal:  J Virol       Date:  2016-06-10       Impact factor: 5.103

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